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Philadelphia positive acute lymphocytic leukaemia – Treatment

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Philadelphia chromosome-positive acute lymphoblastic leukemia (Ph+ ALL) is a specific type of blood cancer that occurs when a genetic mutation creates an abnormal chromosome inside white blood cells. This condition, once considered very difficult to treat, has undergone remarkable transformation in recent years with the introduction of targeted medicines that specifically block the cancer-causing protein produced by this genetic change.

Understanding Treatment Goals in Philadelphia Chromosome-Positive ALL

When someone receives a diagnosis of Philadelphia chromosome-positive acute lymphoblastic leukemia, the primary goal of treatment is to achieve complete remission and ultimately cure the disease. Complete remission means that blast cells—the immature, cancerous white blood cells—are no longer detectable in the blood or bone marrow, and normal blood cell production resumes. However, doctors now aim for an even deeper response called MRD-negative complete remission, where advanced laboratory tests cannot detect any remaining cancer cells, even at a molecular level.[11]

The treatment approach for Ph+ ALL differs significantly from other types of acute lymphoblastic leukemia because of the unique genetic change that drives this disease. This Philadelphia chromosome results from a swap of genetic material between chromosomes 9 and 22, creating a fusion gene called BCR-ABL1. This gene produces an overactive protein that causes white blood cells to multiply uncontrollably.[1]

Treatment strategies depend heavily on several factors, including the patient’s age, overall health, how the disease responds to initial therapy, and whether certain additional genetic changes are present. Doctors monitor response at the molecular level throughout treatment, adjusting medications based on how quickly and completely the BCR-ABL1 protein disappears from the blood and bone marrow.[2]

⚠️ Important
Philadelphia chromosome-positive ALL is more common in older adults, occurring in up to 50% of people over age 50 diagnosed with acute lymphoblastic leukemia. This age-related pattern means treatment plans must often be tailored to accommodate other health conditions and reduced tolerance for intensive chemotherapy in elderly patients.

Standard Treatment Approaches for Ph+ ALL

Before the year 2000, standard treatment for Philadelphia chromosome-positive ALL relied primarily on intensive combination chemotherapy followed by allogeneic stem cell transplantation. Patients treated with chemotherapy alone achieved complete remission rates between 45% and 90%, but most eventually relapsed, and long-term survival remained poor.[1]

The introduction of tyrosine kinase inhibitors (TKIs) revolutionized treatment for Ph+ ALL. These medications specifically target the abnormal BCR-ABL1 protein produced by the Philadelphia chromosome. Imatinib (also known by the brand name Gleevec) was the first tyrosine kinase inhibitor used to treat this disease and became the most widely used TKI when combined with chemotherapy. Clinical trials demonstrated that adding imatinib to chemotherapy regimens produced substantially better outcomes compared to chemotherapy alone.[1]

Current standard treatment typically begins with an induction phase designed to achieve complete remission. This phase combines a tyrosine kinase inhibitor with chemotherapy, though the intensity of chemotherapy used alongside TKIs is generally lower than what was historically used for Ph-negative ALL. The goal during induction is to eliminate detectable leukemia cells from the blood and bone marrow while minimizing treatment-related complications, particularly in older adults who may not tolerate intensive chemotherapy well.[9]

Following successful induction, treatment moves into a consolidation phase. This phase includes continued therapy with TKIs and chemotherapy to deepen and maintain remission. Doctors carefully monitor molecular response by measuring levels of the BCR-ABL1 transcript in blood samples. Achieving complete molecular remission—where BCR-ABL1 becomes undetectable—is a critical milestone that influences decisions about subsequent treatment.[13]

For many years, allogeneic hematopoietic stem cell transplantation (also called allogeneic bone marrow transplant or allo-HCT) during first remission was considered the best option for curing Ph+ ALL. This procedure involves replacing the patient’s diseased bone marrow with healthy stem cells from a matched donor—either a related family member, an unrelated volunteer donor, or a partially matched relative (haploidentical donor). The transplanted cells not only restore normal blood cell production but also provide an immune response against any remaining leukemia cells.[1]

However, transplantation carries significant risks, including graft-versus-host disease (where donated immune cells attack the recipient’s body), infections, and treatment-related mortality. The decision to proceed with transplant depends on multiple factors, including the depth of molecular remission achieved with TKI therapy, the patient’s age and overall health, availability of a suitable donor, and the presence of high-risk genetic features beyond the Philadelphia chromosome.[12]

Side effects of standard treatment vary depending on which medications are used and their intensity. Common side effects of tyrosine kinase inhibitors include fluid retention, muscle cramps, nausea, diarrhea, skin rashes, and fatigue. Imatinib can cause low blood counts, liver function abnormalities, and rarely, heart problems. Chemotherapy side effects include hair loss, increased infection risk due to low white blood cell counts, bleeding risk from low platelets, anemia, mouth sores, and digestive problems. Most side effects resolve after treatment ends, though some may persist long-term.[9]

For patients who undergo stem cell transplantation, TKI therapy is often continued after the procedure as maintenance treatment to prevent relapse. The optimal duration of post-transplant TKI therapy remains an area of ongoing research, with many doctors recommending at least one to two years of continued treatment.[2]

Newer Tyrosine Kinase Inhibitors in Standard Care

While imatinib was the first TKI approved for Ph+ ALL, researchers developed more powerful second-generation and third-generation tyrosine kinase inhibitors that have now become part of standard treatment approaches. Dasatinib is a second-generation TKI that is more potent than imatinib—meaning it can block the BCR-ABL1 protein more effectively and at lower doses. Clinical studies evaluating dasatinib combined with low-intensity chemotherapy or even without chemotherapy have shown promising results, with high rates of complete remission and molecular response.[1]

Another second-generation TKI used in clinical practice is nilotinib, which also demonstrates greater potency than imatinib. Both dasatinib and nilotinib have been incorporated into treatment protocols and may be preferred over imatinib in certain situations, particularly when rapid disease control is essential or when patients develop intolerance to imatinib.[9]

Ponatinib is a third-generation TKI with unique importance in treating Ph+ ALL because it is the only approved tyrosine kinase inhibitor that works against the T315I mutation. This specific mutation can develop in the BCR-ABL1 gene during treatment with other TKIs, causing resistance—meaning the leukemia stops responding to imatinib, dasatinib, or nilotinib. When doctors detect the T315I mutation through genetic testing, switching to ponatinib often restores disease control.[10]

Ponatinib has been evaluated in combination with chemotherapy for newly diagnosed Ph+ ALL patients and has shown excellent results, including high rates of deep molecular remission. However, ponatinib carries specific risks, particularly related to blood vessel problems that can lead to heart attack, stroke, or blood clots. Doctors carefully monitor patients receiving ponatinib and may adjust doses based on response and side effects.[13]

Innovative Treatments Being Tested in Clinical Trials

Clinical research continues to transform the treatment landscape for Philadelphia chromosome-positive ALL. Several promising approaches are currently being studied in clinical trials at medical centers in the United States, Europe, and other regions around the world. These studies test new combinations of drugs, novel targeted therapies, and immunotherapy approaches that harness the immune system to fight leukemia cells.

One of the most exciting developments in recent years involves blinatumomab, a type of immunotherapy called a bispecific T-cell engager. Blinatumomab is not a traditional chemotherapy drug but rather an engineered antibody that simultaneously binds to CD19 (a protein found on B-cell ALL cells) and CD3 (a protein on T cells, a type of immune cell). By connecting leukemia cells directly to T cells, blinatumomab redirects the patient’s own immune system to recognize and destroy the cancer cells.[11]

Clinical trials have explored using blinatumomab in combination with TKIs for newly diagnosed Ph+ ALL, particularly in regimens that reduce or eliminate the need for traditional chemotherapy. Phase 2 studies combining blinatumomab with dasatinib or ponatinib have produced remarkable results, with very high rates of complete remission and molecular response. Some of these studies reported that more than 80-90% of patients achieved MRD-negative complete remission without receiving intensive chemotherapy, which could spare patients from chemotherapy’s significant side effects.[11]

These chemotherapy-free or low-chemotherapy approaches are particularly important for older adults and patients with other medical conditions who cannot tolerate intensive treatment. The combination of TKIs and blinatumomab offers the possibility of achieving deep remissions while maintaining quality of life and reducing treatment-related complications. Trials testing these combinations are ongoing, and preliminary results suggest they may become a new standard of care in the future.[2]

Another monoclonal antibody being studied in clinical trials is inotuzumab ozogamicin. This drug combines an antibody that targets CD22 (another protein on B-cell ALL cells) with a chemotherapy drug that is delivered directly to the cancer cells. Inotuzumab has shown significant activity in relapsed or treatment-resistant Ph+ ALL and is now being tested in earlier lines of treatment, including as part of first-line therapy in combination with TKIs.[12]

Clinical trials are also investigating whether certain patients can safely avoid allogeneic stem cell transplantation if they achieve very deep molecular remissions with these newer treatment combinations. Some studies are testing whether patients who become MRD-negative (no detectable minimal residual disease) early in treatment can be cured with TKI and immunotherapy maintenance alone, without the risks associated with transplantation. This represents a major shift in thinking, as transplant has historically been considered essential for curing Ph+ ALL.[11]

Newer third-generation TKIs beyond ponatinib are also being developed and tested. These include molecules designed to overcome multiple types of resistance mutations and to have fewer side effects, particularly regarding cardiovascular complications. Early-phase clinical trials (Phase 1 and Phase 2) evaluate the safety, optimal dosing, and preliminary effectiveness of these experimental drugs in patients whose disease no longer responds to currently available TKIs.[13]

For patients who experience relapse after initial treatment, clinical trials offer access to several innovative therapies. CAR T-cell therapy is a form of cellular immunotherapy where a patient’s own T cells are collected, genetically engineered to recognize and attack leukemia cells, expanded in the laboratory, and then infused back into the patient. CAR T-cell therapies targeting CD19 or CD22 are being studied for relapsed or refractory Ph+ ALL, though they are not yet standard treatment for this specific subtype.[7]

Patient eligibility for clinical trials typically depends on factors such as disease stage (newly diagnosed, relapsed, or refractory), prior treatments received, overall health status, organ function, and sometimes specific genetic characteristics of the leukemia. Trials are conducted at major cancer centers and academic medical institutions. Patients interested in clinical trials should discuss options with their oncology team, who can help identify appropriate studies and facilitate referral and enrollment.[2]

⚠️ Important
When Ph+ ALL stops responding to treatment, doctors test for ABL mutations—genetic changes in the BCR-ABL1 gene that can cause resistance to tyrosine kinase inhibitors. The T315I mutation is the most common resistance mechanism, and identifying it through molecular testing allows doctors to switch to ponatinib, the only TKI that works against this specific change. Regular monitoring for mutations helps guide treatment adjustments before the disease progresses significantly.

Monitoring Treatment Response and Molecular Testing

Throughout treatment for Ph+ ALL, doctors use sophisticated laboratory tests to monitor how well therapy is working. These tests measure measurable residual disease (MRD), which refers to very small numbers of leukemia cells that may remain in the body even when standard tests show complete remission. MRD testing can detect one leukemia cell among 10,000 to one million normal cells, making it far more sensitive than traditional methods.[2]

The most important molecular test for Ph+ ALL measures levels of the BCR-ABL1 transcript using a technique called RT-qPCR (reverse transcription quantitative polymerase chain reaction). This test detects and quantifies the abnormal BCR-ABL1 RNA in blood or bone marrow samples. Doctors perform this test repeatedly during and after treatment to assess response and detect early signs of relapse. A steadily declining or undetectable BCR-ABL1 level indicates good treatment response, while rising levels may signal disease progression or emergence of drug resistance.[10]

Next-generation sequencing (NGS) represents an even more advanced approach to MRD monitoring. NGS-based tests can detect extremely low levels of disease and identify specific mutations in the ABL gene that confer resistance to particular TKIs. This information helps doctors select the most appropriate TKI if treatment needs to be changed. Some clinical trials now use NGS-based MRD assessment, such as the Clonoseq platform, for precise measurement of disease response.[2]

Additional monitoring includes regular blood counts to assess for recovery of normal blood cell production, bone marrow biopsies at key treatment milestones, and testing for chromosomal abnormalities beyond the Philadelphia chromosome. Some patients with Ph+ ALL have additional high-risk genetic changes, such as deletions affecting a gene called IKZF1 (sometimes called IKZF1-plus). The presence of these additional abnormalities may influence treatment decisions, particularly regarding the need for stem cell transplantation.[13]

Most Common Treatment Methods

  • Tyrosine Kinase Inhibitors (TKIs)
    • Imatinib (first-generation TKI) combined with chemotherapy has been the most widely used approach and significantly improved outcomes compared to chemotherapy alone
    • Dasatinib (second-generation TKI) offers more potent BCR-ABL1 inhibition and is being studied in combination with low-intensity chemotherapy or blinatumomab
    • Ponatinib (third-generation TKI) is the only TKI effective against the T315I mutation and shows excellent results when combined with chemotherapy in newly diagnosed patients
    • TKIs are continued as maintenance therapy after achieving remission and may be used after stem cell transplantation to prevent relapse
  • Chemotherapy
    • Combination chemotherapy regimens using multiple drugs (such as vincristine, daunorubicin, cyclophosphamide, and corticosteroids like prednisone or dexamethasone) to eliminate leukemia cells
    • Less intensive chemotherapy protocols are often used when combined with TKIs, particularly for older patients
    • Chemotherapy intensity has decreased with improved TKI therapy, reducing treatment-related toxicity while maintaining effectiveness
    • Central nervous system prophylaxis with intrathecal chemotherapy (medication injected directly into the spinal fluid) to prevent leukemia spread to the brain and spinal cord
  • Immunotherapy
    • Blinatumomab, a bispecific T-cell engager antibody that connects leukemia cells to immune cells, used for patients with detectable MRD or in combination with TKIs as first-line treatment
    • Inotuzumab ozogamicin, an antibody-drug conjugate targeting CD22, studied in clinical trials for both relapsed disease and upfront treatment
    • These immunotherapy approaches offer alternatives to intensive chemotherapy with different side effect profiles
  • Allogeneic Stem Cell Transplantation
    • Historically considered essential for curing Ph+ ALL during first complete remission
    • Recommended particularly for patients who do not achieve complete molecular remission or who have additional high-risk genetic features
    • Can use stem cells from matched related donors, unrelated volunteer donors, or partially matched family members (haploidentical transplant)
    • The role of transplantation is evolving as newer drug combinations achieve deeper remissions, with some clinical trials exploring whether transplant can be safely omitted for patients achieving early MRD-negative status

Ongoing Clinical Trials on Philadelphia positive acute lymphocytic leukaemia

  • Study of olverembatinib with chemotherapy versus standard therapy in adults with newly diagnosed Philadelphia chromosome-positive acute lymphoblastic leukemia

    Recruiting

    1 1 1 1
    Investigated diseases:
    Investigated drugs:
    Bulgaria Czechia France Hungary Italy Romania +1

  • Study on Ponatinib and Blinatumomab for Adults with Philadelphia Chromosome-Positive Acute Lymphoblastic Leukemia

    Not recruiting

    1 1 1 1
    Investigated diseases:
    Investigated drugs:
    Italy

References

https://pmc.ncbi.nlm.nih.gov/articles/PMC4199301/

https://www.nature.com/articles/s41375-024-02319-2

https://www.cancerresearchuk.org/about-cancer/acute-lymphoblastic-leukaemia-all/about

https://www.medicalnewstoday.com/articles/philadelphia-positive-acute-lymphoblastic-leukemia

https://www.mdanderson.org/cancer-types/acute-lymphocytic-leukemia.html

https://bloodcancer.org.uk/understanding-blood-cancer/leukaemia/acute-lymphoblastic-leukaemia/what-is-all/

https://blog.stbaldricks.org/what-is-philadelphia-chromosome-positive-all/

https://pubmed.ncbi.nlm.nih.gov/40555197/

https://pubmed.ncbi.nlm.nih.gov/30675645/

https://www.iclusig.com/ph-positive-all/understanding-ph-positive-all

https://chi.scholasticahq.com/article/117026-how-i-treat-newly-diagnosed-acute-lymphoblastic-leukemia

https://www.bloodresearch.or.kr/journal/view.html?doi=10.5045/br.2020.S006

https://pmc.ncbi.nlm.nih.gov/articles/PMC10741425/

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Philadelphia positive acute lymphocytic leukaemia:

FAQ

What makes Philadelphia chromosome-positive ALL different from other types of acute lymphoblastic leukemia?

Ph+ ALL is defined by a specific genetic change where parts of chromosomes 9 and 22 swap places, creating the BCR-ABL1 fusion gene that produces an overactive protein causing uncontrolled white blood cell growth. This unique feature allows doctors to use targeted medications called tyrosine kinase inhibitors that specifically block this abnormal protein, making treatment approach and prognosis distinctly different from Philadelphia chromosome-negative ALL.

Will I need a stem cell transplant if I have Ph+ ALL?

Whether you need a stem cell transplant depends on several factors, including how deeply and quickly your disease responds to initial treatment with TKIs and chemotherapy, your age and overall health, the presence of additional high-risk genetic features, and availability of a suitable donor. Historically, transplant was recommended for all Ph+ ALL patients in first remission, but newer treatment combinations achieving very deep molecular responses may allow some patients to avoid transplant. Your doctor will discuss whether transplant is necessary based on your individual disease characteristics and response to treatment.

What happens if my Ph+ ALL stops responding to the tyrosine kinase inhibitor I’m taking?

If your leukemia stops responding to your current TKI (called resistance), your doctor will test for mutations in the BCR-ABL1 gene that may be causing this resistance. The most common resistance mutation is T315I, which makes leukemia cells resistant to imatinib, dasatinib, and nilotinib, but ponatinib can effectively target this mutation. Your treatment may be switched to a different TKI, combined with immunotherapy like blinatumomab, or you may be offered enrollment in a clinical trial testing newer medications. Stem cell transplantation is also an option for patients with resistant disease.

Are there treatment options that don’t require intensive chemotherapy?

Yes, researchers are studying chemotherapy-free or low-intensity chemotherapy approaches for Ph+ ALL. Clinical trials combining tyrosine kinase inhibitors with immunotherapy drugs like blinatumomab have shown that many patients can achieve deep remissions without traditional intensive chemotherapy. These approaches are particularly promising for older adults or patients with other health conditions who may not tolerate intensive chemotherapy well. However, these chemotherapy-free regimens are not yet standard treatment outside of clinical trials, though they may become standard options in the future.

How will my doctor know if treatment is working?

Doctors use multiple tests to monitor treatment response, including regular blood counts, bone marrow examinations, and molecular testing that measures levels of the BCR-ABL1 transcript in your blood or bone marrow. The most important assessment is measuring minimal residual disease (MRD) using highly sensitive techniques that can detect one leukemia cell among hundreds of thousands or millions of normal cells. Achieving MRD-negative status—where these sensitive tests cannot detect any leukemia cells—indicates excellent treatment response and is associated with better long-term outcomes.

🎯 Key Takeaways

  • Philadelphia chromosome-positive ALL, once considered nearly incurable, now has survival rates exceeding 60-70% thanks to targeted therapies called tyrosine kinase inhibitors that specifically block the cancer-causing BCR-ABL1 protein.
  • Treatment typically combines TKIs like imatinib, dasatinib, or ponatinib with less intensive chemotherapy than was historically used, reducing side effects while improving outcomes.
  • Achieving MRD-negative complete remission—where advanced tests cannot detect any remaining cancer cells—is now the primary treatment goal and strongly predicts long-term disease control.
  • Ponatinib is the only TKI that works against the T315I mutation, the most common cause of resistance to other tyrosine kinase inhibitors.
  • Immunotherapy with blinatumomab, which directs the immune system to attack leukemia cells, shows remarkable effectiveness when combined with TKIs and may eliminate the need for intensive chemotherapy in many patients.
  • Clinical trials testing chemotherapy-free combinations of TKIs and immunotherapy are achieving complete remission rates above 90%, potentially revolutionizing how Ph+ ALL is treated.
  • The role of stem cell transplantation is evolving—while historically considered essential, some patients achieving very deep molecular remissions with newer drug combinations may be cured without transplant.
  • Regular molecular monitoring throughout treatment allows doctors to detect early signs of resistance or relapse and adjust therapy before disease progression occurs.

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